We are excited to present our new study combining in vivo CRISPR perturbation sequencing with barcode-based lineage tracing. Our study reveals a mechanism by which selective enhancer activation establishes the identity of GABAergic projection neurons. This work may help to better understand neurologic disease caused by MEIS2 mutations. Thanks to @Elena_dvoretskova, May, Volker, our collaborators, and
biorxiv.org/content/10.1101/20
#ERC

Spatial enhancer activation determines inhibitory neuron identity

The mammalian telencephalon contains a tremendous diversity of GABAergic projection neuron and interneuron types, that originate in a germinal zone of the embryonic basal ganglia. How genetic information in this transient structure is transformed into different cell types is not yet fully understood. Using a combination of in vivo lineage tracing, CRISPR perturbation and ChIP-seq in mice, we found that the transcription factor MEIS2 favors the development of projection neurons through genomic binding sites in regulatory enhancers of projection neuron specific genes. MEIS2 requires the presence of the homeodomain transcription factor DLX5 to direct its functional activity towards these sites. In interneurons, the activation of projection neuron specific enhancers by MEIS2 and DLX5 is repressed by the transcription factor LHX6. When MEIS2 carries a mutation associated with intellectual disability in humans, it is less effective at activating enhancers involved in projection neuron development. This suggests that GABAergic differentiation may be impaired in patients carrying this mutation. Our research has uncovered a mechanism by which the selective activation of enhancers plays a crucial role in the establishment of neuronal identity, as well as in potential pathological mechanisms. ### Competing Interest Statement The authors have declared no competing interest.

www.biorxiv.org

I am very excited to announce that my lab will join the Young Investigator Programme. I am greatly honored to have been selected for this program, and I look forward to interacting with the program's research groups.

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